US20100056843A1 - Brachytherapy Seed With Fast Dissolving Matrix for Optimal Delivery of Radionuclides To Cancer Tissue - Google Patents

Brachytherapy Seed With Fast Dissolving Matrix for Optimal Delivery of Radionuclides To Cancer Tissue Download PDF

Info

Publication number
US20100056843A1
US20100056843A1 US12/202,954 US20295408A US2010056843A1 US 20100056843 A1 US20100056843 A1 US 20100056843A1 US 20295408 A US20295408 A US 20295408A US 2010056843 A1 US2010056843 A1 US 2010056843A1
Authority
US
United States
Prior art keywords
resorbable
seed
beta
polymer matrix
microspheres
Prior art date
Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
Abandoned
Application number
US12/202,954
Inventor
Darrell R. Fisher
You Han Bae
Current Assignee (The listed assignees may be inaccurate. Google has not performed a legal analysis and makes no representation or warranty as to the accuracy of the list.)
Battelle Memorial Institute Inc
University of Utah Research Foundation UURF
University of Utah
Original Assignee
Battelle Memorial Institute Inc
Priority date (The priority date is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the date listed.)
Filing date
Publication date
Application filed by Battelle Memorial Institute Inc filed Critical Battelle Memorial Institute Inc
Priority to US12/202,954 priority Critical patent/US20100056843A1/en
Priority to US12/552,190 priority patent/US8821364B2/en
Priority to BRPI0918594A priority patent/BRPI0918594A2/en
Priority to CA2733823A priority patent/CA2733823C/en
Priority to PCT/US2009/055738 priority patent/WO2010028048A1/en
Priority to CN2009801340864A priority patent/CN102202644A/en
Priority to KR1020117007638A priority patent/KR101660061B1/en
Priority to MX2011002095A priority patent/MX2011002095A/en
Priority to EP09792174.6A priority patent/EP2331064B1/en
Assigned to BATTELLE MEMORIAL INSTITUTE reassignment BATTELLE MEMORIAL INSTITUTE ASSIGNMENT OF ASSIGNORS INTEREST (SEE DOCUMENT FOR DETAILS). Assignors: FISHER, DARRELL R.
Assigned to UNIVERSITY OF UTAH RESEARCH FOUNDATION reassignment UNIVERSITY OF UTAH RESEARCH FOUNDATION ASSIGNMENT OF ASSIGNORS INTEREST (SEE DOCUMENT FOR DETAILS). Assignors: UNIVERSITY OF UTAH
Assigned to UNIVERSITY OF UTAH reassignment UNIVERSITY OF UTAH ASSIGNMENT OF ASSIGNORS INTEREST (SEE DOCUMENT FOR DETAILS). Assignors: BAE, YOU HAN
Publication of US20100056843A1 publication Critical patent/US20100056843A1/en
Priority to CL2011000380A priority patent/CL2011000380A1/en
Priority to CO11040324A priority patent/CO6491121A2/en
Priority to US14/454,605 priority patent/US9289625B2/en
Priority to US15/069,801 priority patent/US20160193479A1/en
Abandoned legal-status Critical Current

Links

Images

Classifications

    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61NELECTROTHERAPY; MAGNETOTHERAPY; RADIATION THERAPY; ULTRASOUND THERAPY
    • A61N5/00Radiation therapy
    • A61N5/10X-ray therapy; Gamma-ray therapy; Particle-irradiation therapy
    • A61N5/1001X-ray therapy; Gamma-ray therapy; Particle-irradiation therapy using radiation sources introduced into or applied onto the body; brachytherapy
    • A61N5/1027Interstitial radiation therapy
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61NELECTROTHERAPY; MAGNETOTHERAPY; RADIATION THERAPY; ULTRASOUND THERAPY
    • A61N5/00Radiation therapy
    • A61N5/10X-ray therapy; Gamma-ray therapy; Particle-irradiation therapy
    • A61N5/1001X-ray therapy; Gamma-ray therapy; Particle-irradiation therapy using radiation sources introduced into or applied onto the body; brachytherapy
    • A61N2005/1019Sources therefor
    • A61N2005/1024Seeds
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61NELECTROTHERAPY; MAGNETOTHERAPY; RADIATION THERAPY; ULTRASOUND THERAPY
    • A61N5/00Radiation therapy
    • A61N5/10X-ray therapy; Gamma-ray therapy; Particle-irradiation therapy
    • A61N2005/1085X-ray therapy; Gamma-ray therapy; Particle-irradiation therapy characterised by the type of particles applied to the patient
    • A61N2005/1089Electrons

Definitions

  • the present invention relates to therapeutic radiology. More particularly, the present invention is directed to radioactive materials contained in polymers for use in therapeutic applications known as brachytherapy.
  • Treatment of cancerous tissue by exposure to radiation-emitting material is now a well established and accepted practice.
  • the aims of such a practice include targeting exposure of radiation to the tissue adjacent to a radiation source while keeping the radiation effects on neighboring healthy tissue to a minimum.
  • a major advantage of this form of treatment is that it concentrates the emitted radiation at the site where the treatment is needed, e.g. within or adjacent to a tumor, while keeping the amount of radiation transmitted to the healthy tissue far below what it otherwise would be if the radiation were beamed into the body from an external source, using other forms of teletherapy.
  • Prior art forms of brachytherapy typically include various processes such as placing the source(s) typically small capsules, approximately 4.5 mm long and 0.8 mm in diameter, called seeds containing a radiation sources such as iodine-125, cesium-131, or palladium-103, which are placed within the tissue to be treated, i.e. interstitial therapy.
  • the capsule is typically designed to allow the rapid and facile insertion of the seed into the organ or body part being treated, with minimal trauma to the surrounding tissue. These devices are many times inserted into the body percutaneously using a hollow needle which is preloaded with the desired number of therapy seeds.
  • a stylet is used to hold the seeds in place while the needle is withdrawn from around them, leaving the seeds in the desired location.
  • encapsulating devices and materials have been utilized and are presently contemplated.
  • these materials contain the radioactive material while allowing photon radiation (Auger x-rays) to irradiate cancerous tissues while the radioactive source decays to negligible activity.
  • the metallic seed remains permanently implanted.
  • a further polymer embodiment containing the radioactive source may gradually dissolve in the body after the radioactive source has decayed to negligible activity.
  • Another major drawback for metal-encapsulated seeds is that the encapsulating metal absorbs a significant fraction of the radiation emitted by the contained radioisotope, for example about 14% of the iodine-125 x-rays and 40% of the palladium-103 x-rays are absorbed in the encapsulating metal in the current commercial seeds.
  • an additional amount of relatively costly radioisotope activity must be added to overcome the losses in the encapsulating metal.
  • the effective thickness of the metal is not the same in all directions resulting in a radiation field around the seed which is not uniform, a fact that complicates treatment planning and raises the possibility of the existence of areas within the treatment volume in which the radiation dose is below that required to kill all tumor cells present.
  • the current practice of brachytherapy based on the use of discrete encapsulated sources is limited by: the need to associate groups of discrete seeds together by some means so that they can be placed into tissue in a predetermined array and held in that array throughout the therapeutic life of the sources, the need for complex treatment planning that takes into account the discrete nature of the seeds and the shape of the radiation field around each seed with the assumption the field shape around each seed is uniformly the same, the need to add excess radioactivity to compensate for the radiation absorption in the encapsulating metal, and the creation of a nonuniform radiation field around the source because the geometry and effective thickness of the encapsulating metal is not the same in all directions, and the radiation field about a source is not spherical.
  • the present invention as disclosed herein, significantly reduces each of these limitations and furthermore allows a more complete realization of the potential benefits of brachytherapy.
  • the present invention includes a device, method and system for implementing brachytherapy and creating devices for use in such methods and systems.
  • the present invention provides substantial advantages over the devices taught in the prior art.
  • the present invention is a method for treating tumor cells utilizing a resorbable therapy seed made up of microspheres containing a beta-particle-emitting radiation source and a resorbable polymer matrix containing the microspheres.
  • these seeds are implanted within the cell and then dissolved or broken so as to release the microspheres.
  • These microspheres then slightly spread within a preselected target area and provide radiation therapy in an amount and at the rate of radioisotope decay according the specific needs and necessities of the users.
  • the configuration of the microspheres, the types of radiation provided and the location and use of these microspheres provide desired localized treatment to target cells while preferentially avoiding undesired damage to surrounding tissue. Because beta radiation is defined by a distinct energy-range cutoff, this method combined with the materials and methods for production of these materials provides a significantly more effective and less expensive therapy alternative than other methods taught in the prior art.
  • the resorbable therapy seed contains a plurality of microspheres preferably of a generally uniform size, and having a diameter of less than 50 microns. While these preferred descriptions are provided it is to be distinctly understood that that the invention is not thereto but may be variously alternatively embodied according the respective needs and necessities of the individual user.
  • Each of these individual microspheres contains a beta particle emitting material such as yttrium-90 preferably bound up in an insoluble chemical form. While yttrium-90 has been provided as an example of one material, it is to be distinctly understood that the invention is not limited thereto but may be variously embodied and configured to include a variety of materials including but not limited to phosphorus-32, copper-64, copper-67, iodine-131, Iutetiumn-177, samarium-153, holmium-166, rhenium-186, and rhenium-188. This chemical binding of radioisotope with-in an insoluble form prevents dissolution and release of the radioactive material in body fluids translocation to other parts of the body where such radiation is not desired. A colloid form of binding while not required is preferable.
  • the resorbable seeds of the present invention also contain an imaging material.
  • imaging materials may be utilized including but not limited to metallic, preferably gold, particles.
  • these microspheres and these imaging materials are mixed within a resorbable polymer matrix that holds the materials together but can respond, after surgical delivery, to various stimuli such as temperature, pH, ultrasonic energy, body fluid characteristics and other influences which increase polymer dissolution rates.
  • This combination can then be extruded into a shape, preferably rods and then and cut into individual seeds of a particular preselected size. These individual seeds can then be coated with a preferably thin, outer coating so as to provide particular advantages consistent with the needs and necessities of the user.
  • the resorbable therapy seed provides a therapeutic index greater than 1.0, and has an effective therapy range that is limited by the range of beta-particles in the seed or target tissue (approximately 1.1 cm for yttrium-90) to limit therapy doses to target tissues within this range and protect normal tissue outside of this range from undesirable radiation effects.
  • the method of the present invention can then be performed.
  • the method comprises the steps of implanting a resorbable therapy seed such as those described above within a preselected tumor or at a preselected location.
  • a resorbable therapy seed such as those described above within a preselected tumor or at a preselected location.
  • imaging of the location of the seed can be accomplished.
  • the seed is dissolved through any of a variety of ways depending upon the particular material that the polymer matrix is composed of. Thus the dissolution of this material may take place through ultrasonic energy, reaction with the internal temperature of the body, reaction with a body fluid or any of a variety of other ways.
  • the radioactive microspheres are appropriately released within the target cancer. These microspheres remain in place and the beta emissions from the microspheres are appropriately delivered to the target tissues.
  • the present invention provides a variety of additional advantages over the prior art. These include but are not limited to better radiation quality for tumor cell killing, a better therapeutic index by reducing the dose to nearby normal tissues, and therefore the ability to treat tumors at higher doses than is taught in the prior art, lower cost for materials and preparation, resorbable seed materials dissolve into the body rather than leaving metal pieces in the body, the provision of an outer thin coating that can be variously configured for alternative embodiments and modalities, the ability of the seed to be degraded by ultrasound, and the prevention of unintended migration of the beta emitting material throughout the body.
  • FIG. 1 is a cut-away view of a first embodiment of the device of the present invention.
  • FIG. 2 a is a photograph of a tumor mass without implanted marker spheres.
  • FIG. 2 b shows directly injected marker spheres in the tumor, imaged by ultrasound to demonstrate marker imageability.
  • FIG. 3 a shows a hypothetical tumor mass within a hypothetical normal mass of tissue
  • FIG. 3 b shows the potential placement of resorbable seeds within the hypothetical tumor mass.
  • FIG. 3 c shows the redistribution of radioactive microspheres after rapid dissolution of the polymer matrix
  • FIG. 3 d shows the effective high radiation field around each grouping of radioactive microspheres with sparing of most of the normal tissue.
  • FIGS. 1-3 show various views and embodiments of the present invention and its implementation.
  • present invention is a bioresorbable, fast-dissolving brachytherapy seed 12 .
  • this seed 12 is configured to resemble traditional generally cylindrical brachytherapy seeds (generally having an overall diameter of about 1 mm or less and an overall length of about 5 mm or less).
  • This seed contains a plurality of microspheres 12 .
  • Each of these microspheres 12 contain a beta particle radiation source 14 which is preferably insolubilized in a colloid formulation so as to prevent the undesired dissolution and movement of these sources away from a desired location after surgical implantation.
  • an imaging marker 16 consisting of metallic markers are also located within the polymer matrix 18 together with the beta particle microspheres 12 are held within a polymer matrix 18 .
  • This polymer matrix 18 is configured to dissolve quickly when subjected to a preselected set of conditions.
  • the imaging material markers 16 and the beta particle containing microspheres 12 migrate to a designated location.
  • the portions of the microsphere 12 that contain the radiation emissions are removed and release of radiation energy within the tumor takes place.
  • the radioactive material from inside the seed 12 to partially redistribute within the tumor.
  • the radioactive source is the beta-emitter yttrium-90, in an insoluble form (phosphate) or colloid, to ensure that the radioactive material does not dissolve in body fluids and redistribute widely throughout the body after release from the resorbable or fast-dissolving seed matrix material 18 . This allows the radioactive source 14 to remain in the tumor for localized radiation therapy.
  • the seed 10 is administered as a solid cylinder by conventional seed-placement mechanisms and grids.
  • the seed 10 also contains imageable markers 16 to allow the surgeon placing the seed to visualize seed placement within the tumor.
  • the fast-dissolving matrix 18 allows beta-emitters to be used with greater flexibility and energy-delivery efficiency than if the radionuclide were to be contained within a slow-dissolving polymer or metallic (non-resorbable) seed exterior. Use of beta-emitting radionuclides with well-defined range and cut-off distance enables a higher dose to be delivered to tumors without exceeding the normal tissue tolerance of surrounding normal tissues and organs for improved tumor-irradiation efficacy.
  • the embodiment of the invention described herein allows delivery of the encased radioactive source material to the tumor without loss by contamination prior to delivery, protects hospital workers and the patient from loose contamination, or spread into the environment as radioactive contamination, rapidly dissolves in the tumor after surgical placement, and can be easily formable into a desired size, (In the preferred embodiment this is generally a cylinder shape with a diameter of 0 . 5 to 0 . 8 mm and a length of about 4.5 to 5 mm).
  • Two different kinds of technology will be employed for extruding or pressing the seed, however it is to be distinctly understood that the invention is not limited thereto but may be variously embodied according to the needs and necessities of a user.
  • a wet granule preparation process is utilized.
  • all seed materials including the radioactive source 14 , gold markers 16 , and rapidly dissolving excipients 18-mixed together with proper solvents are combined for form a mixture.
  • This mixture is then extruded against a desired size sieve and dried in an oven. These extruded sections can then be cut into seeds of a desired size and if desired coated with a coating material 20 .
  • the second method for preparing the brachytherapy granules involves directly compressing the seeds from the mixture of radiation source 14 , imaging materials 16 , and polymer matrix 18 , using a mini seed or granule-making machine. This direct compression method is generally preferred, however if the mixed material is powder and difficult to prepare to make granules by direct compression method, the previously described wet method will be the preferred alternative.
  • the matrix 18 containing the radioactive source 14 and marker material 16 dissolve quickly (minutes to hours) to release the radioactive source 14 in tumor tissue after placement. This is dramatically shorter than prior art seeds which typically require weeks to months to dissolve.
  • the dissolution of the polymer matrix 18 can be variously configured according to the needs of the user. Various types of stimuli can be utilized to accomplish this dissolution including but not limited to heat, ultrasound, body fluid, and other stimuli. Similar types of stimuli can be utilized to affect the coating 20 of the seed.
  • the polymer matrix 18 is one that disintegrates rapidly in water or body fluids.
  • the polymer-matrix 18 is a temperature-induced or thermally stimulated, rapidly dissolving system.
  • a beta-particle-emitting radionuclide such as yttrium-90, rhenium-186, rhenium-188, or Iutetium-177 is utilized as insoluble colloid or microsphere 12 .
  • These seeds 10 also may contain markers such as radioactive gold-198 or gold-197, or with stable gold markers.
  • These formulations will serve as brachytherapy and position-monitoring source materials for imaging—for example by ultrasound or gamma-camera imaging system common to nuclear medicine clinics.
  • dissolution of the polymer matrices may be enhanced by the user of 1 to 3 MHz ultrasound on the site of tumor after localizing the seeds 10 to enhance break-up of the and dissolution of the seed matrix.
  • a water or body fluid dissolvable polymer matrix 18 includes crospovidone(N-vinyl-2-pyrrolidone) sold under the trade name Polyplasdone® XL-10, International Specialty Products Wayne, N.J. USA.
  • crospovidone N-vinyl-2-pyrrolidone
  • Polyplasdone® XL-10 International Specialty Products Wayne, N.J. USA.
  • other materials include but are not limited to polyvinylpyrrolidone, starch, algirlic acid, formaldehyde, calcium carboxymethyl cellulose, sodium starch glycolate, and sodium carboxymethyl cellulose.
  • cellulose derivatives may also serve as an excipient.
  • hydroxypropylmethylcellulose such as those sold under the trade names “TC-5E”, “Metolose 90”, “Metolose 65SH”, trade names; produced by Shin-Etsu Chemical Co., Ltd. Tokyo, Japan
  • hydroxypropylcellulose for example, “Nisso HPC”, trade name; produced by Nippon Soda Co., Ltd. Tokyo, Japan
  • methyl cellulose for example, “Metolose SM”, trade name; produced by Shin-Etsu Chemical Co., Ltd., Tokyo, Japan
  • NATROSOL hydroxyethylcellulose
  • More preferred is hydroxypropylmethylcellulose.
  • soluble diluents agents may be required for the wet prepping process of the invention these include but are not limited to a soluble diluent with binding properties that consist of a polyol having less than 13 carbon atoms and being either in the form of the directly compressible product with an average particle diameter of 100 to 500 micrometers, or in the form of a powder with an average particle diameter of less than 100 micrometers.
  • this polyol is selected from the group comprising mannitol, xylitol, sorbitol and maltitol.
  • the addition of a lubricant used in the fast release formulation may also be utilized.
  • lubricants examples include conventional lubricants, such as magnesium stearate, sodium dodecyl sulfate. Generally, it is preferred that the lubricant be water soluble. Hence, the preferred lubricant is sodium dodecyl sulfate in an amount ranging from about 1 to 3 percent.
  • the polymer based matrix is a temperature-sensitive rapid disintegrating formulation.
  • Temperature-sensitive, rapid-dissolving formulations are preferably made from materials that are in a generally solid state at room temperature and provide sufficient rigidity to allow injection of a seed made from such material into the tumor tissue. This material preferably would then dissolve in the tumor site at 37-42 degrees C. Ultrasound treatment can be used to increase local material temperature.
  • Formulation matrices can be oleophilic bases and/or water-soluble bases, and can be used in combination. Examples of oleophilic bases include cacao butter, lanolin fat and hard fats.
  • hard fats examples include: Witepsol, tradename, manufactured by Huls Inc.), Suppocire, tradename, (manufactured by Gattefosse Inc.), lsocacao, tradename, (manufactured by Kao Corp.), and tradename, Pharmasol (manufactured by NOF Corp.), etc.
  • the beta emitting radiation source has a generally short half-life (less than 60 days, and preferably less than 9 days). More specifically, in certain cases the radioisotope is selected from the group of of yttrium-90, phosphorus-32, copper-64, copper-67, iodine-131, Iutetium-177, samarium-153, holmium-166, rhenium-186, rhenium-188, and combinations thereof. Beta particles have short path length in tissue, which indicates minimal irradiation of surrounding normal tissue. In addition, these beta emitting radiation sources are generally confined to a specific target tissue.
  • the purpose of the radioactive confine is to minimize or prevent migration of the radioisotope to healthy tissue areas.
  • the confined radioisotope may be confined, for example, by chelators or complexing agents, capsules, and combinations thereof.
  • useful isotope/chelator combinations are, for example, yttrium-90 with 1,4,7,10-tetraazacyclododecane-N,N′,N′′,N′′′-tetraacetic acid (DOTA), derivatives of DOTA.
  • insoluble salts such as 90-yttrium phosphate may also be utilized. It is preferred that particles of the insoluble salt are hydrothermally synthesized in solution as the disperse phase of a colloid.
  • a colloid is a chemical system composed of a continuous medium (continuous phase) throughout which are distributed small particles, for example about 0.0001 micrometer to about 3 micrometer in size (the disperse phase).
  • Hydrothermal synthesis refers to the synthesis of products by reacting reagents in solution at temperatures and/or pressures above ambient temperature and/or pressure, such as by performing the reaction in a sealed vessel (generally known as a hydrothermal bomb) that may also be heated.
  • the hydrothermal bomb may include a liner in which reagents are reacted so that the bomb can more easily be reused.
  • Hydrothermal synthesis of insoluble salt particles allows for control of particle shape and/or size. While uniform size and shape are not required, these characteristics can aid in determining the amount of radioactive agent to administer to achieve a particular dosage of radiation to tissue in vivo. That is the more uniform the particles are in size and/or shape the more consistent the radiation doses for a particular amount of particles because similar sized and/or shaped particles provide similar amounts of radiation.
  • hydrothermal syntheses of insoluble salt radioactive therapeutic agents include a complexing agent, such as a compound comprising ethylene diamine tetraacetic acid (EDTA), to bind metal cations, such as Y.sup.3+, in solution, allowing the cations to exceed the saturation concentration without significant precipitation of the salt.
  • EDTA ethylene diamine tetraacetic acid
  • the EDTA releases the cations to react with anions, such as YPO.sub.4.sup.3 ⁇ , to form particles.
  • the particles formed are colloidal, that is, the particles form a disperse phase of a colloid in the continuous phase of the solution.
  • colloids including YPO.sub.4 particles as the disperse phase are synthesized using EDTA, an yttrium (Y) source, and a phosphate (PO.sub.4) source, all reacted in a hydrothermal bomb.
  • EDTA EDTA
  • Y yttrium
  • PO.sub.4 phosphate
  • the seeds in the preferred embodiment also include an imaging material such as a metallic marking material.
  • an imaging material such as a metallic marking material.
  • gold particles were utilized as an ultrasound marker or contrast agent. The presence of these marking materials allows placement of the seeds in the tissue to be verified and monitored through the use of ultrasound imaging. Examples of such images are shown in FIG. 2 a - b.
  • FIG. 2 a shows a tumor ultrasound images before marker placement
  • FIG. 2 b shows a tumor ultrasound image after placement of spherical markers into a mouse tumor.
  • this material when combined with the seed matrix, could render the brachytherapy seeds sufficiently imageable via ultrasound for practical application as an aid to surgical placement in tumor tissue.
  • ultrasound imaging is described herein it is to be distinctly understood that the imaging step is not limited thereto but may be variously embodied and configured according to the needs and necessities of the user.
  • ultrasound may also be used to enhance matrix dissolution This can be done utilizing a device such as a Omnisound 3000 commercialized ultrasound machine with 1 MHz and 3 MHz signals, that modify the power density, duty cycle, and wave irradiation time to optimize the brachytherapy seed dissolution.
  • a device such as a Omnisound 3000 commercialized ultrasound machine with 1 MHz and 3 MHz signals, that modify the power density, duty cycle, and wave irradiation time to optimize the brachytherapy seed dissolution.
  • a seeds 12 as described above are implanted into a selected portion of tumor tissue.
  • the tumor is preferably imaged to verify placement of the seeds in the desired location. After this imaging has taken place, the seeds are dissolved and microparticles that contain the beta-emitting source are then released to provide therapeutic radiation to the tumor to destroy the unwanted tumor tissue.
  • this method provides several advantages. First, this method provides a user the ability to use inexpensive materials as the seed matrix, radioisotope, and markers. Second, this less expensive seed has the ability to deliver higher localized radiation doses to radiation-insensitive solid tumors (which could include cancers of the liver, pancreas, brain, head and neck, prostate, colon, and others, or solid tumors that are not resectable and that must be treated effectively without surgical removal, such as those that may surround the vocal chords or spinal column nerves.
  • the present invention provides an ability to use radioisotopes other than the more common Auger-electron-emitters traditionally used in seed brachytherapy, such as iodine-125, paladium-103, and cesium-131, which are all relatively expensive to produce.
  • the present invention also provides the ability to deliver more locally intense radiation doses to tumor tissues than achieved using the Auger-electron emitters mentioned above. While various preferred embodiments of the invention are shown and described, it is to be distinctly understood that this invention is not limited thereto but may be variously embodied to practice within the scope of the following claims. From the foregoing description, it will be apparent that various changes may be made without departing from the spirit and scope of the invention as defined by the following claims.

Abstract

A system, method and device for treating tumor cells utilizing a resorbable therapy seed made up of microspheres containing a beta-particle-emitting radiation source and a resorbable polymer matrix. These seeds are implanted within the tumor and then rapidly dissolved or broken so as to release the microspheres. These microspheres then spread within a preselected target area and provide radiation therapy in a predetermined amount and at a preselected rate according the specific needs and necessities of the users. The configuration of the microspheres, the types of radiation provided and the location and use of these microspheres provides desired localized treatment to target cells while preferentially avoiding undesired damage to surrounding tissue. The present invention provides a method for making the seeds, as well as a method for utilizing the seeds as a part of the treatment method.

Description

    FIELD OF THE INVENTION
  • The present invention relates to therapeutic radiology. More particularly, the present invention is directed to radioactive materials contained in polymers for use in therapeutic applications known as brachytherapy.
    • BACKGROUND OF THE INVENTION
  • Treatment of cancerous tissue by exposure to radiation-emitting material is now a well established and accepted practice. Generally, the aims of such a practice include targeting exposure of radiation to the tissue adjacent to a radiation source while keeping the radiation effects on neighboring healthy tissue to a minimum. A major advantage of this form of treatment is that it concentrates the emitted radiation at the site where the treatment is needed, e.g. within or adjacent to a tumor, while keeping the amount of radiation transmitted to the healthy tissue far below what it otherwise would be if the radiation were beamed into the body from an external source, using other forms of teletherapy.
  • Prior art forms of brachytherapy typically include various processes such as placing the source(s) typically small capsules, approximately 4.5 mm long and 0.8 mm in diameter, called seeds containing a radiation sources such as iodine-125, cesium-131, or palladium-103, which are placed within the tissue to be treated, i.e. interstitial therapy. In various embodiments of the construction, the capsule is typically designed to allow the rapid and facile insertion of the seed into the organ or body part being treated, with minimal trauma to the surrounding tissue. These devices are many times inserted into the body percutaneously using a hollow needle which is preloaded with the desired number of therapy seeds. When the needle is in the desired location in the tissue, a stylet is used to hold the seeds in place while the needle is withdrawn from around them, leaving the seeds in the desired location. The use of such small radiation sources is a common way of practicing interstitial brachytherapy.
  • In many such methods it is typically considered necessary and in some cases crucial to enclose the radioactive material with an encapsulating material so as to contain the radioactive material and preventing it from becoming systemically distributed within the patient or escaping into the environment where it could contaminate medical personnel, medical facilities or the general environment.
  • Various types of encapsulating devices and materials have been utilized and are presently contemplated. Typically these materials contain the radioactive material while allowing photon radiation (Auger x-rays) to irradiate cancerous tissues while the radioactive source decays to negligible activity. Typically, the metallic seed remains permanently implanted. A further polymer embodiment containing the radioactive source may gradually dissolve in the body after the radioactive source has decayed to negligible activity.
  • Another major drawback for metal-encapsulated seeds is that the encapsulating metal absorbs a significant fraction of the radiation emitted by the contained radioisotope, for example about 14% of the iodine-125 x-rays and 40% of the palladium-103 x-rays are absorbed in the encapsulating metal in the current commercial seeds. As a consequence, to obtain the desired radiation dose rate on the exterior of the seed, an additional amount of relatively costly radioisotope activity must be added to overcome the losses in the encapsulating metal. Also, because it is typically necessary to seal (or weld) the ends of the capsules, the effective thickness of the metal is not the same in all directions resulting in a radiation field around the seed which is not uniform, a fact that complicates treatment planning and raises the possibility of the existence of areas within the treatment volume in which the radiation dose is below that required to kill all tumor cells present.
  • Thus the current practice of brachytherapy based on the use of discrete encapsulated sources is limited by: the need to associate groups of discrete seeds together by some means so that they can be placed into tissue in a predetermined array and held in that array throughout the therapeutic life of the sources, the need for complex treatment planning that takes into account the discrete nature of the seeds and the shape of the radiation field around each seed with the assumption the field shape around each seed is uniformly the same, the need to add excess radioactivity to compensate for the radiation absorption in the encapsulating metal, and the creation of a nonuniform radiation field around the source because the geometry and effective thickness of the encapsulating metal is not the same in all directions, and the radiation field about a source is not spherical. The present invention as disclosed herein, significantly reduces each of these limitations and furthermore allows a more complete realization of the potential benefits of brachytherapy. The present invention includes a device, method and system for implementing brachytherapy and creating devices for use in such methods and systems. The present invention provides substantial advantages over the devices taught in the prior art.
  • Additional advantages and novel features of the present invention will be set forth as follows and will be readily apparent from the descriptions and demonstrations set forth herein. Accordingly, the following descriptions of the present invention should be seen as illustrative of the invention and not as limiting in any way.
    • SUMMARY
  • The present invention is a method for treating tumor cells utilizing a resorbable therapy seed made up of microspheres containing a beta-particle-emitting radiation source and a resorbable polymer matrix containing the microspheres. In use, these seeds are implanted within the cell and then dissolved or broken so as to release the microspheres. These microspheres then slightly spread within a preselected target area and provide radiation therapy in an amount and at the rate of radioisotope decay according the specific needs and necessities of the users. The configuration of the microspheres, the types of radiation provided and the location and use of these microspheres provide desired localized treatment to target cells while preferentially avoiding undesired damage to surrounding tissue. Because beta radiation is defined by a distinct energy-range cutoff, this method combined with the materials and methods for production of these materials provides a significantly more effective and less expensive therapy alternative than other methods taught in the prior art.
  • In one embodiment of the invention the resorbable therapy seed contains a plurality of microspheres preferably of a generally uniform size, and having a diameter of less than 50 microns. While these preferred descriptions are provided it is to be distinctly understood that that the invention is not thereto but may be variously alternatively embodied according the respective needs and necessities of the individual user.
  • Each of these individual microspheres contains a beta particle emitting material such as yttrium-90 preferably bound up in an insoluble chemical form. While yttrium-90 has been provided as an example of one material, it is to be distinctly understood that the invention is not limited thereto but may be variously embodied and configured to include a variety of materials including but not limited to phosphorus-32, copper-64, copper-67, iodine-131, Iutetiumn-177, samarium-153, holmium-166, rhenium-186, and rhenium-188. This chemical binding of radioisotope with-in an insoluble form prevents dissolution and release of the radioactive material in body fluids translocation to other parts of the body where such radiation is not desired. A colloid form of binding while not required is preferable.
  • This beta emitting material is then encapsulated by a fast-resorbable polymer that acts to give physical form to the brachytherapy seed, enable surgical placement, and restrain the beta particle emitting material in a desired position and location. In addition to these microspheres, the resorbable seeds of the present invention also contain an imaging material. Various examples of imaging materials may be utilized including but not limited to metallic, preferably gold, particles. Preferably, these microspheres and these imaging materials are mixed within a resorbable polymer matrix that holds the materials together but can respond, after surgical delivery, to various stimuli such as temperature, pH, ultrasonic energy, body fluid characteristics and other influences which increase polymer dissolution rates. This combination can then be extruded into a shape, preferably rods and then and cut into individual seeds of a particular preselected size. These individual seeds can then be coated with a preferably thin, outer coating so as to provide particular advantages consistent with the needs and necessities of the user.
  • Preferably, the resorbable therapy seed provides a therapeutic index greater than 1.0, and has an effective therapy range that is limited by the range of beta-particles in the seed or target tissue (approximately 1.1 cm for yttrium-90) to limit therapy doses to target tissues within this range and protect normal tissue outside of this range from undesirable radiation effects.
  • With these seeds, the method of the present invention can then be performed. In one embodiment of the invention the method comprises the steps of implanting a resorbable therapy seed such as those described above within a preselected tumor or at a preselected location. Once surgically placed, if desired, imaging of the location of the seed can be accomplished. After the seed has been placed, it is dissolved through any of a variety of ways depending upon the particular material that the polymer matrix is composed of. Thus the dissolution of this material may take place through ultrasonic energy, reaction with the internal temperature of the body, reaction with a body fluid or any of a variety of other ways. Once the seed polymer encapsulation has been appropriately placed and dissolved, the radioactive microspheres are appropriately released within the target cancer. These microspheres remain in place and the beta emissions from the microspheres are appropriately delivered to the target tissues.
  • The present invention provides a variety of additional advantages over the prior art. These include but are not limited to better radiation quality for tumor cell killing, a better therapeutic index by reducing the dose to nearby normal tissues, and therefore the ability to treat tumors at higher doses than is taught in the prior art, lower cost for materials and preparation, resorbable seed materials dissolve into the body rather than leaving metal pieces in the body, the provision of an outer thin coating that can be variously configured for alternative embodiments and modalities, the ability of the seed to be degraded by ultrasound, and the prevention of unintended migration of the beta emitting material throughout the body.
  • The purpose of the foregoing abstract is to enable the United States Patent and Trademark Office and the public generally, especially the scientists, engineers, and practitioners in the art who are not familiar with patent or legal terms or phraseology, to determine quickly from a cursory inspection the nature and essence of the technical disclosure of the application. The abstract is neither intended to define the invention of the application, which is measured by the claims, nor is it intended to be limiting as to the scope of the invention in any way.
  • Various advantages and novel features of the present invention are described herein and will become further readily apparent to those skilled in this art from the following detailed description. In the preceding and following descriptions I have shown and described only the preferred embodiment of the invention, by way of illustration of the best mode contemplated for carrying out the invention. As will be realized, the invention is capable of modification in various respects without departing from the invention. Accordingly, the drawings and description of the preferred embodiment set forth hereafter are to be regarded as illustrative in nature, and not as restrictive.
    • BRIEF DESCRIPTION OF THE DRAWINGS
  • FIG. 1 is a cut-away view of a first embodiment of the device of the present invention.
  • FIG. 2 a is a photograph of a tumor mass without implanted marker spheres.
  • FIG. 2 b shows directly injected marker spheres in the tumor, imaged by ultrasound to demonstrate marker imageability.
  • FIG. 3 a shows a hypothetical tumor mass within a hypothetical normal mass of tissue
  • FIG. 3 b shows the potential placement of resorbable seeds within the hypothetical tumor mass.
  • FIG. 3 c shows the redistribution of radioactive microspheres after rapid dissolution of the polymer matrix
  • FIG. 3 d shows the effective high radiation field around each grouping of radioactive microspheres with sparing of most of the normal tissue.
    •  DETAILED DESCRIPTION OF THE INVENTION
  • The following description includes the preferred best mode of one embodiment of the present invention. It will be clear from this description of the invention that the invention is not limited to these illustrated embodiments but that the invention also includes a variety of modifications and embodiments thereto. Therefore the present description should be seen as illustrative and not limiting. While the invention is susceptible of various modifications and alternative constructions, it should be understood, that there is no intention to limit the invention to the specific form disclosed, but, on the contrary, the invention is to cover all modifications, alternative constructions, and equivalents falling within the spirit and scope of the invention as defined in the claims.
  • FIGS. 1-3 show various views and embodiments of the present invention and its implementation. Referring now to FIG. 1, one embodiment of the device of the present invention is shown. In this embodiment of the invention, present invention is a bioresorbable, fast-dissolving brachytherapy seed 12. In this embodiment this seed 12 is configured to resemble traditional generally cylindrical brachytherapy seeds (generally having an overall diameter of about 1 mm or less and an overall length of about 5 mm or less). This seed contains a plurality of microspheres 12. Each of these microspheres 12 contain a beta particle radiation source 14 which is preferably insolubilized in a colloid formulation so as to prevent the undesired dissolution and movement of these sources away from a desired location after surgical implantation. In this preferred embodiment an imaging marker 16 consisting of metallic markers are also located within the polymer matrix 18 together with the beta particle microspheres 12 are held within a polymer matrix 18. This polymer matrix 18 is configured to dissolve quickly when subjected to a preselected set of conditions.
  • Once the seed 10 has been placed and the polymer matrix 18 has been dissolved, the imaging material markers 16 and the beta particle containing microspheres 12 migrate to a designated location. The portions of the microsphere 12 that contain the radiation emissions are removed and release of radiation energy within the tumor takes place. This allows the radioactive material from inside the seed 12 to partially redistribute within the tumor. In one embodiment, the radioactive source is the beta-emitter yttrium-90, in an insoluble form (phosphate) or colloid, to ensure that the radioactive material does not dissolve in body fluids and redistribute widely throughout the body after release from the resorbable or fast-dissolving seed matrix material 18. This allows the radioactive source 14 to remain in the tumor for localized radiation therapy.
  • In this preferred embodiment of the invention, the seed 10 is administered as a solid cylinder by conventional seed-placement mechanisms and grids. The seed 10 also contains imageable markers 16 to allow the surgeon placing the seed to visualize seed placement within the tumor. The fast-dissolving matrix 18 allows beta-emitters to be used with greater flexibility and energy-delivery efficiency than if the radionuclide were to be contained within a slow-dissolving polymer or metallic (non-resorbable) seed exterior. Use of beta-emitting radionuclides with well-defined range and cut-off distance enables a higher dose to be delivered to tumors without exceeding the normal tissue tolerance of surrounding normal tissues and organs for improved tumor-irradiation efficacy.
  • The embodiment of the invention described herein allows delivery of the encased radioactive source material to the tumor without loss by contamination prior to delivery, protects hospital workers and the patient from loose contamination, or spread into the environment as radioactive contamination, rapidly dissolves in the tumor after surgical placement, and can be easily formable into a desired size, (In the preferred embodiment this is generally a cylinder shape with a diameter of 0.5 to 0.8 mm and a length of about 4.5 to 5 mm). Two different kinds of technology will be employed for extruding or pressing the seed, however it is to be distinctly understood that the invention is not limited thereto but may be variously embodied according to the needs and necessities of a user.
  • In one method of preparing the seeds, a wet granule preparation process is utilized. In this embodiment all seed materials, including the radioactive source 14, gold markers 16, and rapidly dissolving excipients 18-mixed together with proper solvents are combined for form a mixture. This mixture is then extruded against a desired size sieve and dried in an oven. These extruded sections can then be cut into seeds of a desired size and if desired coated with a coating material 20. The second method for preparing the brachytherapy granules involves directly compressing the seeds from the mixture of radiation source 14, imaging materials 16, and polymer matrix 18, using a mini seed or granule-making machine. This direct compression method is generally preferred, however if the mixed material is powder and difficult to prepare to make granules by direct compression method, the previously described wet method will be the preferred alternative.
  • In this preferred embodiment of the present invention the matrix 18 containing the radioactive source 14 and marker material 16 dissolve quickly (minutes to hours) to release the radioactive source 14 in tumor tissue after placement. This is dramatically shorter than prior art seeds which typically require weeks to months to dissolve. The dissolution of the polymer matrix 18 can be variously configured according to the needs of the user. Various types of stimuli can be utilized to accomplish this dissolution including but not limited to heat, ultrasound, body fluid, and other stimuli. Similar types of stimuli can be utilized to affect the coating 20 of the seed.
  • In one preferred embodiment of the invention the polymer matrix 18 is one that disintegrates rapidly in water or body fluids. In another embodiment of the invention the polymer-matrix 18 is a temperature-induced or thermally stimulated, rapidly dissolving system. In either of these embodiments a beta-particle-emitting radionuclide, such as yttrium-90, rhenium-186, rhenium-188, or Iutetium-177 is utilized as insoluble colloid or microsphere 12. These seeds 10 also may contain markers such as radioactive gold-198 or gold-197, or with stable gold markers. These formulations will serve as brachytherapy and position-monitoring source materials for imaging—for example by ultrasound or gamma-camera imaging system common to nuclear medicine clinics. In some other embodiments and applications dissolution of the polymer matrices may be enhanced by the user of 1 to 3 MHz ultrasound on the site of tumor after localizing the seeds 10 to enhance break-up of the and dissolution of the seed matrix.
  • In a preferred formulation a water or body fluid dissolvable polymer matrix 18 includes crospovidone(N-vinyl-2-pyrrolidone) sold under the trade name Polyplasdone® XL-10, International Specialty Products Wayne, N.J. USA. In addition to this material, a variety of other types of materials may also be utilized to bring about a similar result. Examples of such other materials include but are not limited to polyvinylpyrrolidone, starch, algirlic acid, formaldehyde, calcium carboxymethyl cellulose, sodium starch glycolate, and sodium carboxymethyl cellulose.
  • In addition to these materials, cellulose derivatives may also serve as an excipient. These include hydroxypropylmethylcellulose, such as those sold under the trade names “TC-5E”, “Metolose 90”, “Metolose 65SH”, trade names; produced by Shin-Etsu Chemical Co., Ltd. Tokyo, Japan), hydroxypropylcellulose (for example, “Nisso HPC”, trade name; produced by Nippon Soda Co., Ltd. Tokyo, Japan), methyl cellulose (for example, “Metolose SM”, trade name; produced by Shin-Etsu Chemical Co., Ltd., Tokyo, Japan), and hydroxyethylcellulose (“NATROSOL”, trade name; produced by Hercules Japan, Ltd., Tokyo Japan). More preferred is hydroxypropylmethylcellulose.
  • Various soluble diluents agents may be required for the wet prepping process of the invention these include but are not limited to a soluble diluent with binding properties that consist of a polyol having less than 13 carbon atoms and being either in the form of the directly compressible product with an average particle diameter of 100 to 500 micrometers, or in the form of a powder with an average particle diameter of less than 100 micrometers. Preferably, this polyol is selected from the group comprising mannitol, xylitol, sorbitol and maltitol. In addition to these materials, the addition of a lubricant used in the fast release formulation may also be utilized. Examples of such lubricants include conventional lubricants, such as magnesium stearate, sodium dodecyl sulfate. Generally, it is preferred that the lubricant be water soluble. Hence, the preferred lubricant is sodium dodecyl sulfate in an amount ranging from about 1 to 3 percent.
  • In a second embodiment of the present invention the polymer based matrix is a temperature-sensitive rapid disintegrating formulation. Temperature-sensitive, rapid-dissolving formulations are preferably made from materials that are in a generally solid state at room temperature and provide sufficient rigidity to allow injection of a seed made from such material into the tumor tissue. This material preferably would then dissolve in the tumor site at 37-42 degrees C. Ultrasound treatment can be used to increase local material temperature. Formulation matrices can be oleophilic bases and/or water-soluble bases, and can be used in combination. Examples of oleophilic bases include cacao butter, lanolin fat and hard fats. Examples of the hard fats include: Witepsol, tradename, manufactured by Huls Inc.), Suppocire, tradename, (manufactured by Gattefosse Inc.), lsocacao, tradename, (manufactured by Kao Corp.), and tradename, Pharmasol (manufactured by NOF Corp.), etc.
  • Preferably the beta emitting radiation source has a generally short half-life (less than 60 days, and preferably less than 9 days). More specifically, in certain cases the radioisotope is selected from the group of of yttrium-90, phosphorus-32, copper-64, copper-67, iodine-131, Iutetium-177, samarium-153, holmium-166, rhenium-186, rhenium-188, and combinations thereof. Beta particles have short path length in tissue, which indicates minimal irradiation of surrounding normal tissue. In addition, these beta emitting radiation sources are generally confined to a specific target tissue.
  • The purpose of the radioactive confine is to minimize or prevent migration of the radioisotope to healthy tissue areas. The confined radioisotope may be confined, for example, by chelators or complexing agents, capsules, and combinations thereof. Examples of useful isotope/chelator combinations are, for example, yttrium-90 with 1,4,7,10-tetraazacyclododecane-N,N′,N″,N′″-tetraacetic acid (DOTA), derivatives of DOTA. In addition to these materials insoluble salts such as 90-yttrium phosphate may also be utilized. It is preferred that particles of the insoluble salt are hydrothermally synthesized in solution as the disperse phase of a colloid. As used herein a colloid is a chemical system composed of a continuous medium (continuous phase) throughout which are distributed small particles, for example about 0.0001 micrometer to about 3 micrometer in size (the disperse phase). Hydrothermal synthesis refers to the synthesis of products by reacting reagents in solution at temperatures and/or pressures above ambient temperature and/or pressure, such as by performing the reaction in a sealed vessel (generally known as a hydrothermal bomb) that may also be heated. The hydrothermal bomb may include a liner in which reagents are reacted so that the bomb can more easily be reused.
  • Hydrothermal synthesis of insoluble salt particles allows for control of particle shape and/or size. While uniform size and shape are not required, these characteristics can aid in determining the amount of radioactive agent to administer to achieve a particular dosage of radiation to tissue in vivo. That is the more uniform the particles are in size and/or shape the more consistent the radiation doses for a particular amount of particles because similar sized and/or shaped particles provide similar amounts of radiation.
  • Certain embodiments of hydrothermal syntheses of insoluble salt radioactive therapeutic agents, such as YPO.sub.4 particles, include a complexing agent, such as a compound comprising ethylene diamine tetraacetic acid (EDTA), to bind metal cations, such as Y.sup.3+, in solution, allowing the cations to exceed the saturation concentration without significant precipitation of the salt. During hydrothermal synthesis the EDTA releases the cations to react with anions, such as YPO.sub.4.sup.3−, to form particles. In certain embodiments the particles formed are colloidal, that is, the particles form a disperse phase of a colloid in the continuous phase of the solution.
  • In certain embodiments, colloids including YPO.sub.4 particles as the disperse phase are synthesized using EDTA, an yttrium (Y) source, and a phosphate (PO.sub.4) source, all reacted in a hydrothermal bomb. A detailed description of such a process is found in US Patent Application Publication 20040228794A1 the contents of which are herein incorporated by reference.
  • Preferably the seeds in the preferred embodiment also include an imaging material such as a metallic marking material. In one preferred embodiment gold particles were utilized as an ultrasound marker or contrast agent. The presence of these marking materials allows placement of the seeds in the tissue to be verified and monitored through the use of ultrasound imaging. Examples of such images are shown in FIG. 2 a-b. FIG. 2 a shows a tumor ultrasound images before marker placement, and FIG. 2 b shows a tumor ultrasound image after placement of spherical markers into a mouse tumor. Thus this material when combined with the seed matrix, could render the brachytherapy seeds sufficiently imageable via ultrasound for practical application as an aid to surgical placement in tumor tissue.
  • While ultrasound imaging is described herein it is to be distinctly understood that the imaging step is not limited thereto but may be variously embodied and configured according to the needs and necessities of the user.
  • If necessary, ultrasound may also be used to enhance matrix dissolution This can be done utilizing a device such as a Omnisound 3000 commercialized ultrasound machine with 1 MHz and 3 MHz signals, that modify the power density, duty cycle, and wave irradiation time to optimize the brachytherapy seed dissolution.
  • In one example of the present invention, a seeds 12 as described above are implanted into a selected portion of tumor tissue. The tumor is preferably imaged to verify placement of the seeds in the desired location. After this imaging has taken place, the seeds are dissolved and microparticles that contain the beta-emitting source are then released to provide therapeutic radiation to the tumor to destroy the unwanted tumor tissue.
  • This method provides several advantages. First, this method provides a user the ability to use inexpensive materials as the seed matrix, radioisotope, and markers. Second, this less expensive seed has the ability to deliver higher localized radiation doses to radiation-insensitive solid tumors (which could include cancers of the liver, pancreas, brain, head and neck, prostate, colon, and others, or solid tumors that are not resectable and that must be treated effectively without surgical removal, such as those that may surround the vocal chords or spinal column nerves. The present invention provides an ability to use radioisotopes other than the more common Auger-electron-emitters traditionally used in seed brachytherapy, such as iodine-125, paladium-103, and cesium-131, which are all relatively expensive to produce. The present invention also provides the ability to deliver more locally intense radiation doses to tumor tissues than achieved using the Auger-electron emitters mentioned above. While various preferred embodiments of the invention are shown and described, it is to be distinctly understood that this invention is not limited thereto but may be variously embodied to practice within the scope of the following claims. From the foregoing description, it will be apparent that various changes may be made without departing from the spirit and scope of the invention as defined by the following claims.

Claims (24)

1. A resorbable therapy seed comprising:
at least two microspheres each containing a beta-particle-emitting radiation source; and a resorbable polymer matrix containing said microspheres.
2. The resorbable therapy seed of claim 1 further comprising a thin protective coating over said resorbable polymer matrix.
3. The resorbable therapy seed of claim 1 further comprising an imaging material.
4. The resorbable therapy seed of claim 3 wherein said imaging material includes a metallic marking material.
5. The resorbable therapy seed of claim 4 wherein said metallic marking material includes microspheres having a diameter less than 50 microns.
6. The resorbable therapy seed of claim 1 wherein said beta-emitting source is bound as an insoluble material within said microsphere.
7. The resorbable therapy seed of claim 1 wherein said resorbable polymer matrix is capable of dissolution by ultrasonic energy.
8. The resorbable therapy seed of claim 1 wherein said beta-emitting source is selected from the group consisting of yttrium-90, phosphorus-32, copper-64, copper-67, iodine-131, Iutetium-177, samarium-153, holmium-166, rhenium-186, rhenium-188, and combinations thereof.
9. The resorbable therapy seed of claim 1 wherein said therapy seed provides a therapeutic index greater than 1.0.
10. The resorbable therapy seed of claim 1 further comprising an imaging material comprising metallic microspheres and a coating over said seed wherein said beta-emitting source is bound as an insoluble material to prevent movement of said radioactive source beyond a preselected target location.
11. The resorbable therapy seed of claim 10 wherein said resorbable polymer matrix is capable of dissolution by ultrasonic energy.
12. The resorbable therapy seed of claim 10 wherein said resorbable polymer matrix is capable of dissolution by body fluids.
13. The resorbable therapy seed of claim 10 wherein said resorbable polymer matrix is capable of dissolution by the natural temperature of the body relative to room temperature.
14. The resorbable therapy seed of claim 10 wherein said beta emitting source is selected from the group consisting of yttrium 90, phosphorus-32, copper-64, copper-67, iodine-131, Iutetium-177, samarium-153, holmium-166, rhenium-186, and rhenium-188.
15. A method for manufacturing resorbable therapy seeds characterized by the step of:
mixing preselected quantities of a beta emitting source in a resorbable matrix-forming polymer material.
16. The method of claim 14 wherein said mixing step further comprises mixing an imaging material with said beta-emitting source and said resorbable matrix-forming polymer material.
17. The method of claim 15 further comprising the step of extruding a mixture of said beta emitting source said resorbable matrix polymer material into rods.
18. The method of claim 16 further comprising the step of cutting said extruded mixture into seed pieces having a preselected size.
19. The method of claim 17 further comprising the step of coating said seed pieces having a preselected size.
20. A method for treating a tumor characterized by the step of:
implanting a resorbable therapy seed having a microspherical particles having a beta-emitting source within a resorbable polymer matrix within a tumor.
21. The method of claim 20 further comprising the step of breaking said polymer matrix using ultrasonic energy.
22. The method of claim 20 further comprising the step of dissolving said polymer matrix using body fluids.
23. The method of claim 20 further comprising the step of dissolving said polymer matrix using body temperature?
24. The method of claim 20 wherein said resorbable therapy seed further comprises an imaging media and wherein said method further comprises the step of imaging said tumor to verify placement of said seeds prior to breaking said polymer matrix using ultrasonic energy and body fluids.
US12/202,954 2008-09-02 2008-09-02 Brachytherapy Seed With Fast Dissolving Matrix for Optimal Delivery of Radionuclides To Cancer Tissue Abandoned US20100056843A1 (en)

Priority Applications (13)

Application Number Priority Date Filing Date Title
US12/202,954 US20100056843A1 (en) 2008-09-02 2008-09-02 Brachytherapy Seed With Fast Dissolving Matrix for Optimal Delivery of Radionuclides To Cancer Tissue
US12/552,190 US8821364B2 (en) 2008-09-02 2009-09-01 Brachytherapy seed with fast dissolving matrix for optimal delivery of radionuclides to cancer tissue
KR1020117007638A KR101660061B1 (en) 2008-09-02 2009-09-02 Brachytherapy seed with fast dissolving matrix for optimal delivery of radionuclides to cancer tissue
EP09792174.6A EP2331064B1 (en) 2008-09-02 2009-09-02 Brachytherapy seed with fast dissolving matrix for optimal delivery of radionuclides to cancer tissue
CA2733823A CA2733823C (en) 2008-09-02 2009-09-02 Brachytherapy seed with fast dissolving matrix for optimal delivery of radionuclides to cancer tissue
PCT/US2009/055738 WO2010028048A1 (en) 2008-09-02 2009-09-02 Brachytherapy seed with fast dissolving matrix for optimal delivery of radionuclides to cancer tissue
CN2009801340864A CN102202644A (en) 2008-09-02 2009-09-02 Brachytherapy seed with fast dissolving matrix for optimal delivery of radionuclides to cancer tissue
BRPI0918594A BRPI0918594A2 (en) 2008-09-02 2009-09-02 fast dissolving matrix brachytherapy seed for optimal radionuclide distribution to cancerous tissue
MX2011002095A MX2011002095A (en) 2008-09-02 2009-09-02 Brachytherapy seed with fast dissolving matrix for optimal delivery of radionuclides to cancer tissue.
CL2011000380A CL2011000380A1 (en) 2008-09-02 2011-02-22 Granule to be used in brachytherapy, comprising an insoluble or colloidal structure with radioisotope, a resorbable polymer matrix, which in turn comprises individual particles, consisting of sorbitol coated with a biodegradable polymer; and method for manufacturing said granules.
CO11040324A CO6491121A2 (en) 2008-09-02 2011-04-01 SEEDS FOR BRAQUITERAPY WITH QUICK DISSOLVING MATRIX FOR AN OPTIMAL SUPPLY OF RADIONUCLEID TO CANCEROSE TISSUE
US14/454,605 US9289625B2 (en) 2008-09-02 2014-08-07 Brachytherapy seed with fast dissolving matrix for optimal delivery of radionuclides to cancer tissue
US15/069,801 US20160193479A1 (en) 2008-09-02 2016-03-14 Brachytherapy Seed with Fast Dissolving Matrix for Optimal Delivery of Radionuclides to Cancer Tissue

Applications Claiming Priority (1)

Application Number Priority Date Filing Date Title
US12/202,954 US20100056843A1 (en) 2008-09-02 2008-09-02 Brachytherapy Seed With Fast Dissolving Matrix for Optimal Delivery of Radionuclides To Cancer Tissue

Related Child Applications (1)

Application Number Title Priority Date Filing Date
US12/552,190 Continuation-In-Part US8821364B2 (en) 2008-09-02 2009-09-01 Brachytherapy seed with fast dissolving matrix for optimal delivery of radionuclides to cancer tissue

Publications (1)

Publication Number Publication Date
US20100056843A1 true US20100056843A1 (en) 2010-03-04

Family

ID=41726409

Family Applications (1)

Application Number Title Priority Date Filing Date
US12/202,954 Abandoned US20100056843A1 (en) 2008-09-02 2008-09-02 Brachytherapy Seed With Fast Dissolving Matrix for Optimal Delivery of Radionuclides To Cancer Tissue

Country Status (1)

Country Link
US (1) US20100056843A1 (en)

Cited By (5)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US20120123189A1 (en) * 2009-08-06 2012-05-17 Koninklijke Philips Electronics N.V. Oncology therapies employing radioactive seeds
WO2014145397A1 (en) * 2013-03-15 2014-09-18 Herskovic Arnold M Device and method for delivering medicaments
WO2015057530A3 (en) * 2013-10-15 2015-10-29 Ip Liberty Vision Corporation Radioactive epoxy in ophthalmic brachytherapy
WO2022130195A1 (en) * 2020-12-16 2022-06-23 Alpha Tau Medical Ltd. Diffusing alpha-emitters radiation therapy with enhanced beta treatment
WO2022198100A1 (en) * 2021-03-19 2022-09-22 Gt Medical Technologies, Inc. Systems and methods for creating custom brachytherapy carriers

Citations (5)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US20030088140A1 (en) * 2001-11-02 2003-05-08 Terwilliger Richard A. Delivery system and method for interstitial radiation therapy
US6589502B1 (en) * 1995-11-27 2003-07-08 International Brachytherapy S.A. Radioisotope dispersed in a matrix for brachytherapy
US6746661B2 (en) * 2000-11-16 2004-06-08 Microspherix Llc Brachytherapy seed
US20040197264A1 (en) * 2003-04-04 2004-10-07 Alexander Schwarz Microspheres comprising therapeutic and diagnostic radioactive isotopes
US20060269587A1 (en) * 1999-01-29 2006-11-30 Avi Biopharma, Inc. Antisense restenosis composition and method

Patent Citations (5)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US6589502B1 (en) * 1995-11-27 2003-07-08 International Brachytherapy S.A. Radioisotope dispersed in a matrix for brachytherapy
US20060269587A1 (en) * 1999-01-29 2006-11-30 Avi Biopharma, Inc. Antisense restenosis composition and method
US6746661B2 (en) * 2000-11-16 2004-06-08 Microspherix Llc Brachytherapy seed
US20030088140A1 (en) * 2001-11-02 2003-05-08 Terwilliger Richard A. Delivery system and method for interstitial radiation therapy
US20040197264A1 (en) * 2003-04-04 2004-10-07 Alexander Schwarz Microspheres comprising therapeutic and diagnostic radioactive isotopes

Cited By (8)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US20120123189A1 (en) * 2009-08-06 2012-05-17 Koninklijke Philips Electronics N.V. Oncology therapies employing radioactive seeds
US8827884B2 (en) * 2009-08-06 2014-09-09 Koninklijke Philips N.V. Oncology therapies employing radioactive seeds
WO2014145397A1 (en) * 2013-03-15 2014-09-18 Herskovic Arnold M Device and method for delivering medicaments
US10420956B2 (en) 2013-03-15 2019-09-24 Boston Scientific Corporation Device and method for delivering medicaments
WO2015057530A3 (en) * 2013-10-15 2015-10-29 Ip Liberty Vision Corporation Radioactive epoxy in ophthalmic brachytherapy
US9827444B2 (en) 2013-10-15 2017-11-28 Ip Liberty Vision Corporation Radioactive epoxy in ophthalmic brachytherapy
WO2022130195A1 (en) * 2020-12-16 2022-06-23 Alpha Tau Medical Ltd. Diffusing alpha-emitters radiation therapy with enhanced beta treatment
WO2022198100A1 (en) * 2021-03-19 2022-09-22 Gt Medical Technologies, Inc. Systems and methods for creating custom brachytherapy carriers

Similar Documents

Publication Publication Date Title
US9289625B2 (en) Brachytherapy seed with fast dissolving matrix for optimal delivery of radionuclides to cancer tissue
US6986880B2 (en) Polymeric-matrix brachytherapy sources
US4702228A (en) X-ray-emitting interstitial implants
US8827884B2 (en) Oncology therapies employing radioactive seeds
US20020103410A1 (en) Methods and implants for providing radiation to a patient
US10646724B2 (en) Brachytherapy devices and related methods having microencapsulated brachytherapy materials
WO1997019706A9 (en) Radioisotope dispersed in a matrix for brachytherapy
US20030092958A1 (en) Delivery system and method for interstitial radiation therapy using seed elements with ends having one of projections and indentations
US20080004483A1 (en) Biodegradable seed placement device and method
US20100056843A1 (en) Brachytherapy Seed With Fast Dissolving Matrix for Optimal Delivery of Radionuclides To Cancer Tissue
CA2577665C (en) Plastic brachytherapy sources
Azhdarinia et al. Regional radiochemotherapy using in situ hydrogel
US6120540A (en) Radio prosthesis
Turrel et al. Techniques of afterloading iridium‐192 interstitial brachytherapy in veterinary medicine
Costa et al. Brazilian demand for iodine-125 seeds in cancer treatment after a decade of medical procedures
US20230181790A1 (en) Radioactive shear thinning biomaterial composition and methods for use
Pathak Use of Radiation in Therapy
Rostelato BRAZILIAN DEMAND FOR I TREATMENT AFTER A DECA

Legal Events

Date Code Title Description
AS Assignment

Owner name: UNIVERSITY OF UTAH,UTAH

Free format text: ASSIGNMENT OF ASSIGNORS INTEREST;ASSIGNOR:BAE, YOU HAN;REEL/FRAME:023516/0477

Effective date: 20081016

Owner name: UNIVERSITY OF UTAH RESEARCH FOUNDATION,UTAH

Free format text: ASSIGNMENT OF ASSIGNORS INTEREST;ASSIGNOR:UNIVERSITY OF UTAH;REEL/FRAME:023516/0480

Effective date: 20081016

Owner name: BATTELLE MEMORIAL INSTITUTE,WASHINGTON

Free format text: ASSIGNMENT OF ASSIGNORS INTEREST;ASSIGNOR:FISHER, DARRELL R.;REEL/FRAME:023517/0160

Effective date: 20081006

STCB Information on status: application discontinuation

Free format text: ABANDONED -- FAILURE TO RESPOND TO AN OFFICE ACTION